Lack of Antinociceptive Cross-Tolerance With Co-Administration of Morphine and Fentanyl Into the Periaqueductal Gray of Male Sprague-Dawley Rats

Bobeck, Erin N.; Schoo, Shauna M.; Ingram, Susan; Morgan, Michael M.

doi:10.1016/j.jpain.2019.03.002

Cited by 12 publications

(7 citation statements)

References 46 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…In the present study, we observed that when morphine pretreated mice were challenged with either fentanyl or morphine, the degree of cross tolerance to fentanyl was less than the tolerance to morphine itself. A similar reduced level of cross tolerance between fentanyl and morphine has been reported in studies of rodent locomotor activity (Brase, ) and antinociception (Bobeck, Schoo, Ingram, & Morgan, ; Paronis & Holzman, ), although one study has reported equal cross tolerance between morphine and fentanyl on antinociception (Romero, Miranda, & Puig, ). Cross tolerance develops between drugs acting at the same receptor, but the degree of cross tolerance will depend upon agonist intrinsic efficacy.…”

Section: Discussionsupporting

confidence: 67%

Fentanyl depression of respiration: Comparison with heroin and morphine

Hill

Santhakumar

Dewey

et al. 2019

British J Pharmacology

138

119

View full text Add to dashboard Cite

Background and Purpose: Fentanyl overdose deaths have reached "epidemic" levels in North America. Death in opioid overdose invariably results from respiratory depression. In the present work, we have characterized how fentanyl depresses respiration, and by comparing fentanyl with heroin and morphine, the active breakdown product of heroin, we have sought to determine the factors, in addition to high potency, that contribute to the lethality of fentanyl.Experimental Approach: Respiration (rate and tidal volume) was measured in awake, freely moving mice by whole body plethysmography.Key Results: Intravenously administered fentanyl produced more rapid depression of respiration than equipotent doses of heroin or morphine. Fentanyl depressed both respiratory rate and tidal volume. Fentanyl did not depress respiration in μ-opioid receptor knockout mice. Naloxone, the opioid antagonist widely used to treat opioid overdose, reversed the depression of respiration by morphine more readily than that by fentanyl, whereas diprenorphine, a more lipophilic antagonist, was equipotent in reversing fentanyl and morphine depression of respiration. Prolonged treatment with morphine induced tolerance to respiratory depression, but the degree of cross tolerance to fentanyl was less than the tolerance to morphine itself. Conclusion and Implications:We propose that several factors (potency, rate of onset, lowered sensitivity to naloxone, and lowered cross tolerance to heroin) combine to make fentanyl more likely to cause opioid overdose deaths than other commonly abused opioids. Lipophilic antagonists such as diprenorphine may be better antidotes than naloxone to treat fentanyl overdose.

show abstract

Section: Discussionsupporting

confidence: 67%

Fentanyl depression of respiration: Comparison with heroin and morphine

Hill

Santhakumar

Dewey

et al. 2019

British J Pharmacology

138

119

View full text Add to dashboard Cite

show abstract

“…Even though morphine and fentanyl are two of the most commonly used opioids to treat pain, morphine and fentanyl appear to engage different signalling pathways when microinjected into the periaqueductal gray (PAG). Antinociception produced by PAG morphine administration has a slower onset and longer duration than fentanyl (Bobeck, McNeal, & Morgan, ), is disrupted by blocking G‐protein signalling by administration of pertussis toxin whereas fentanyl antinociception is not (Bobeck, Ingram, Hermes, Aicher, & Morgan, ; Bodnar, Paul, Rosenblum, Liu, & Pasternak, ), and does not show cross‐tolerance to fentanyl following repeated PAG microinjections (Bobeck, Haseman, Hong, Ingram, & Morgan, ; Bobeck, Schoo, Ingram, & Morgan, ). These differences between morphine and fentanyl could be caused by selective activation of distinct signalling pathways or selective activation of pre‐ or postsynaptic MORs.…”

Section: Introductionmentioning

confidence: 99%

Differences in antinociceptive signalling mechanisms following morphine and fentanyl microinjections into the rat periaqueductal gray

Morgan

Tran

Wescom

et al. 2019

European Journal of Pain

Self Cite

View full text Add to dashboard Cite

Background Morphine and fentanyl are two of the most commonly used opioids to treat pain. Although both opioids produce antinociception by binding to mu‐opioid receptors (MOR), they appear to act via distinct signalling pathways. Objective This study will reveal whether differences in morphine and fentanyl antinociception are the result of selective activation of G‐protein signalling and/or selective activation of pre‐ or postsynaptic MORs. Methods The contribution of each mechanism to morphine and fentanyl antinociception was assessed by microinjecting drugs to alter G‐protein signalling or block potassium channels linked to pre‐ and postsynaptic MORs in the ventrolateral periaqueductal gray (PAG) of male Sprague‐Dawley rats. Results Both morphine and fentanyl produced a dose‐dependent antinociception when microinjected into the PAG. Enhancement of intracellular G‐protein signalling by microinjection of the Regulator of G‐protein Signalling 4 antagonist CCG‐63802 into the PAG enhanced the antinociceptive potency of morphine, but not fentanyl. Microinjection of α‐dendrotoxin into the PAG to block MOR activation of presynaptic Kv+ channels caused a significant rightward shift in the dose–response curve of both morphine and fentanyl. Microinjection of tertiapin‐Q to block MOR activation of postsynaptic GIRK channels caused a larger shift in the dose–response curve for fentanyl than morphine antinociception. Conclusions These findings reveal different PAG signalling mechanisms for morphine and fentanyl antinociception. In contrast with fentanyl, the antinociceptive effects of morphine are mediated by G‐protein signalling primarily activated by presynaptic MORs. Significance Microinjection of the opioids morphine and fentanyl into the periaqueductal gray (PAG) produce antinociception via mu‐opioid receptor signalling. This study reveals differences in the signalling mechanisms underlying morphine and fentanyl antinociception in the PAG. In contrast with fentanyl, morphine antinociception is primarily mediated by presynaptic opioid receptors and is enhanced by blocking RGS proteins.

show abstract

“…The reinforcing effects of fentanyl increase in morphine-withdrawn rats, reflected by a rightward shift of the fentanyl dose-response curve with an increase in maximal effectiveness, whereas the reinforcing effects of fentanyl decrease in opioid-dependent rats [ 33 ]. However, no antinociceptive cross-tolerance occurs with repeated microinjections of morphine and fentanyl into the ventrolateral periaqueductal gray, which may be attributable to the different signaling mechanisms that mediate morphine- and fentanyl-induced antinociception [ 34 , 35 ].…”

Section: Fentanyl Abuse and Withdrawalmentioning

confidence: 99%

Unique Pharmacology, Brain Dysfunction, and Therapeutic Advancements for Fentanyl Misuse and Abuse

et al. 2022

View full text Add to dashboard Cite

Fentanyl is a fully synthetic opioid with analgesic and anesthetic properties. It has become a primary driver of the deadliest opioid crisis in the United States and elsewhere, consequently imposing devastating social, economic, and health burdens worldwide. However, the neural mechanisms that underlie the behavioral effects of fentanyl and its analogs are largely unknown, and approaches to prevent fentanyl abuse and fentanyl-related overdose deaths are scarce. This review presents the abuse potential and unique pharmacology of fentanyl and elucidates its potential mechanisms of action, including neural circuit dysfunction and neuroinflammation. We discuss recent progress in the development of pharmacological interventions, anti-fentanyl vaccines, anti-fentanyl/heroin conjugate vaccines, and monoclonal antibodies to attenuate fentanyl-seeking and prevent fentanyl-induced respiratory depression. However, translational studies and clinical trials are still lacking. Considering the present opioid crisis, the development of effective pharmacological and immunological strategies to prevent fentanyl abuse and overdose are urgently needed.

show abstract

Lack of Antinociceptive Cross-Tolerance With Co-Administration of Morphine and Fentanyl Into the Periaqueductal Gray of Male Sprague-Dawley Rats

Cited by 12 publications

References 46 publications

Fentanyl depression of respiration: Comparison with heroin and morphine

Fentanyl depression of respiration: Comparison with heroin and morphine

Differences in antinociceptive signalling mechanisms following morphine and fentanyl microinjections into the rat periaqueductal gray

Unique Pharmacology, Brain Dysfunction, and Therapeutic Advancements for Fentanyl Misuse and Abuse

Contact Info

Product

Resources

About